1 KDIGO Controversies Conference on Glomerular Diseases Breakout Group Questions November 16-19, 2017 Singapore Group 1: General Principles, Membranoproliferative GN (MPGN), C3 Glomerulonephritis (C3GN) 1. General principles (I) • What constitutes the optimal target blood pressure, lipid levels, fluid and dietary sodium intake in glomerular disease? Is there a best way to choose the type of RAS blockade (ACE inhibitor or ARB, or in combination), diuretics and their dosage in patients with glomerular disease? How are these drugs best adjusted in the presence of nephrotic syndrome and/or progressive decline in GFR? Is there an order that is preferable in terms of the introduction of antihypertensive agents beyond RAS blockade and diuretics? • Are there specific indications where RAAS blockade should not be considered for glomerular disease? Role of an apparent fall in GFR after RAAS blockade: good or bad (correcting hyperfiltration vs. AKI)? When and how should we introduce the “sick day “concept to withholding RAS blockade? Should there be a low GFR cut-off for discontinuing RAAS blockade? Should RAAS blockade be started and up-titrated in patients who have or develop hypotension during treatment? In patients with persistent high-grade proteinuria, should RAAS blockers be increased above the maximum daily dose that is recommended for hypertension? Is there any evidence that RAAS blockade may reduce proteinuria but mask ongoing inflammation in glomerular diseases when immunosuppression is contemplated or being used? (discussions on RAAS blockade should include agents such as direct renin
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KDIGOControversiesConferenceonGlomerularDiseasesBreakoutGroupQuestions
November16-19,2017
SingaporeGroup1:GeneralPrinciples,MembranoproliferativeGN(MPGN),C3Glomerulonephritis(C3GN)1. Generalprinciples(I)
• Whatconstitutestheoptimaltargetbloodpressure,lipidlevels,fluidanddietarysodiumintakeinglomerulardisease?IsthereabestwaytochoosethetypeofRASblockade(ACEinhibitororARB,orincombination),diureticsandtheirdosageinpatientswithglomerulardisease?Howarethesedrugsbestadjustedinthepresenceofnephroticsyndromeand/orprogressivedeclineinGFR?IsthereanorderthatispreferableintermsoftheintroductionofantihypertensiveagentsbeyondRASblockadeanddiuretics?
• AretherespecificindicationswhereRAASblockadeshouldnotbeconsideredforglomerulardisease?RoleofanapparentfallinGFRafterRAASblockade:goodorbad(correctinghyperfiltrationvs.AKI)?Whenandhowshouldweintroducethe“sickday“concepttowithholdingRASblockade?ShouldtherebealowGFRcut-offfordiscontinuingRAASblockade?ShouldRAASblockadebestartedandup-titratedinpatientswhohaveordevelophypotensionduringtreatment?Inpatientswithpersistenthigh-gradeproteinuria,shouldRAASblockersbeincreasedabovethemaximumdailydosethatisrecommendedforhypertension?IsthereanyevidencethatRAASblockademayreduceproteinuriabutmaskongoinginflammationinglomerulardiseaseswhenimmunosuppressioniscontemplatedorbeingused?(discussionsonRAASblockadeshouldincludeagentssuchasdirectrenin
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inhibitors,mineralocorticoidblockers,andepithelialsodiumchannelblockade)
• Whatotherlifestylemodifications(e.g.,diet,exercise,sleephealth,tobacco
use)aregenerallyadvisable?WhatisthepotentialmechanismbywhichobesitycontributestoCKDandinparticularglomerulardiseasepathogenesisandprogression?Whatmedicationsshouldbeconsidered(e.g.,vitaminD,statinsandSGLTinhibitors)beyondRASblockers?Whatshouldbeavoided(e.g.,non-dihydropyridinecalciumchannelblockers)?
• Whatareclinicallyrelevantendpointsforglomerulardiseases?(should
address/commentonbiomarkersingeneralincludingmarkersoftubulardamage)Whataretheimportantaspectsofstudydesigninglomerulardiseasewithrespecttotheregulatoryapprovaldecision-makingprocess?Whichmethodofmonitoringproteinuriashouldbeusedintherapeuticdecisionmakinginclinicalpractice?Shouldhematuriabeusedasamarkerofdiseaseactivityand/orasurrogateendpoint?Ifsoinwhichspecificdiseasesshoulditbemeasuredandhow(i.e.,morphologyexamination;semiquantitativevs.quantitative)?
• Whatistheevidencethatthereisacontributionofbirthweightand/ornephronmasstothepathogenesisandprogressionofglomerulardisease?
• Isthereastandardapproachwhichcouldorshouldbeappliedtobothdevelopedanddevelopingcountriesdespiteresourcelimitationsinthediagnosisandtreatmentofglomerulardisease?
2. Nephroticsyndrome
• Isthereatimetointroduceprophylacticanticoagulanttherapyandifsofor
howlong,andwhichdrugsshouldbeused?(doseadjustmentnecessaryby
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GFR?)Doestheapproachinmembranousnephropathy(MN)differfromotherglomerulardiseasesassociatedwiththenephroticsyndrome?
• Whatistheoptimalapproachtotreatinghyperlipidemia?Whatshouldbethegoal?Whataretherecommendationsoftheuseofprophylaxis(e.g.,forinfections,gastrointestinalbleeding,osteoporosis)inpatientsbeingtreatedwithimmunosuppression?Whataretherecommendationsinregardstothetimingandtypeofvaccinationsinpatientswithglomerulardisease?
3. MPGN(i):ExplainthatMPGNisapatternofinjuryratherthanadiseaseentity.
IsthedivisioninthehistologicclassificationofMPGNintoimmunecomplex-mediatedandcomplement-mediatedGNsufficient?Whatisthelikelihoodofoverlapandisthisdependentontiming(trajectory)orpresumedetiologicaltype?Ifso,whatshouldbethesequenceandlimitofdiagnosticinvestigationinclinicalpractice?Aretherearespecificmonitoringtoolsandifso,inwhichspecificvariants?Inwhichcasesshouldpronaseimmunofluorescenceofkidneybiopsytissuebeperformed?
4. MPGN(ii):Howshouldparaprotein-associatedMPGN(“monoclonalgammopathyofrenalsignificance”)beevaluated?Whatistheapproachtotherapybasedonthisworkup?Whataremeaningfulclinicalendpointsinthisdisease?
5. MPGN(iii):WhatistheappropriateworkupforothervariantsofMPGN,particularinso-calledidiopathicMPGN,andshouldothertypesofdepositiondiseasesuchasfibrillaryandimmunotactoidGNbeincluded?Whichofthesevariantsrequireimmunosuppressivetherapy,andwhatshouldbeusedasclinicallymeaningfulendpointsfortreatment(e.g.,proteinuria/changeinGFR)?Whatistheevidencetosupportimmunosuppressivetherapyhere?Whatistheapproachtothediagnosis,treatmentandmonitoringofhepatitisC-associatedglomerulonephritis?
6. MPGN(iv):Incomplementassociated/mediatedMPGN,howspecificallycandysregulationofthedifferentcomplementpathways(classic,lectin,alternate)bedemonstrated,andcanthisinformtheuseanddevelopmentofcomplement
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inhibitorsforthesediseases?WhatistheroleofeculizumabinC3G?Whereareweinthedevelopmentofadditionalcomplementinhibitorstoday?Wheredotheyactinthecomplementcascadeandistherelikelytobespecificityofthesedrugsinrelationshiptospecificcomplementassociated/MPGNvariants?WhatisthedistinctioninC3dominantinfection-associatedGN?Aretherespecialconsiderationsinthepre-andpost-transplantmanagementofpatientswithESKDduetoMPGN/C3glomerulopathy?
Group2:IgANephropathy(IgAN)
Pathogenesis1. Aretherenewinsightsintopathogenesisthatcanguidetreatment?
Biomarkers&predictionofprognosis2. Whichclinical,laboratoryandpathologicparametersshouldformthebasisfor
riskassessment?Shouldmicrohematuria(qualitativeorquantitative?)beincorporatedintheriskassessment?
3. Whatistheroleofnewbiomarkers,suchassCD89andtransferrinreceptor?4. IstherearapidlyprogressivelyGN(RPGN)variantofIgANoristhissevere
hypertensiveinjury(withorwithoutthromboticmicroangiopathy)superimposedonIgAN?
5. Shouldpathology,inparticulartheOxford-MEST-Cclassification,guide
treatment?Howdocrescentsaffecttreatmentdecisions?Aretherehistologicalthresholdsthatcanguidetreatment?
6. InIgAvasculitis,aretherebiomarkersofrenalinvolvementandprognosis?
Shouldaseparatehistologicalclassificationbeconsidered?
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Treatment7. Whatistheevidencesuggestingrenalbenefitatareasonablecost-benefitratio
ofestablishedimmunosuppressivemono-orcombination-therapy(suchassteroids,mycophenolatemofetil,cyclophosphamide,azathioprine)?Andwhatistheoptimumdosage,dosingintervals,durationoftreatmentanddrugformulationforsteroiduseinIgAN?
8. WhatmaybetheimmunosuppressivestrategyinpatientswithlowerGFRs?Is
therea"pointofnoreturn"forIgAN?Ifso,whatisitintermsofeGFR?9. Howshouldonetreatrelapsesofproteinuriafollowinganinitialresponseto
therapy(i.e.,supportiveorimmunosuppressive)?10. HowshouldonemanagenephroticpatientswithIgANwithoutfeaturesof
minimalchangedisease(MCD)inthekidneybiopsy?11. Shouldethnicityinfluencetreatmentdecision?12. Istherearolefortonsillectomy?Futurestudies13. Aretherenovelemergingimmunosuppressiveorotherapproaches(suchas
rituximab,tacrolimus,entericcorticosteroids,BAFFinhibitor,MASP2antibodyandACTH)toprogressiveIgAN?
14. WhatisthefutureofclinicaltrialsinIgAN?
• Howcanclinicaltrialsbefacilitatedinthefuture?• Inclusionofhigh-riskpatientsonly?• Appropriateendpoints?• Determiningoptimaltimeforassessingprimaryendpoint
Durationofclinicaltrial/follow-up
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• Patientreportedoutcomemeasures&sideeffects
Optionalquestionstoaddress(subjecttoavailabilityoftimesinceevidencefromtheliteratureforthesetopicsistooscarcetowarrantincorporationintoaguideline)
1. WhatistheroleofcomplementinhibitioninIgAN?
2. WhatistheroleofthegutmicrobiomeinIgAN,andhowmaydietaryorothertherapiesaffectthisrelationship?Whatistheroleofgluten-freedietinlightofanRCTofgluten-freedietbeingplannedinItaly?
3. HowshouldonemanageIgANinthepediatricpopulation?
4. HowshouldonemanagerecurrentIgANinthekidneytransplantrecipient?
5. HowshouldonemanagepregnancyinpatientswithIgAN?
6. Canweformulaterecommendationsthatshouldbe“standard-of-care”(SOC)inallregionsandhighlightalternativeapproachesthatmaybeexchangedforSOCinresource-limitedcountries?
Group3:MembranousGN(MGN)
Diagnosis1. CanadiagnosisofMNbemadereliablywithoutkidneybiopsy?
2. Isakidneybiopsyneededbeforestartofimmunosuppressivetherapy?
3. IsPLA2R(antibodiesorinbiopsy)sufficienttoruleoutsecondaryMN?What
shouldbethealgorithmforcancerscreening?
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Biomarkers&predictionofprognosis4. Whichclinicalandlaboratoryparameterspredictspontaneousremission?
5. Doantibodyassays(PLA2R,THSD7A)contributetopredictionofspontaneous
remission?Shouldqualitativeassaysbereplacedbyquantitativeassays?Areepitope-specificassayspreferable?
Treatment6. Howshouldremissionbedefined?
a. Arethecurrentdefinitionsofpartialremissionandcompleteremissionappropriate?Couldtheybeimproved?
b. Howshouldanti-PLA2Rbeintegratedintothesedefinitions?c. Shouldothermarkersbeincluded?
7. Whatshouldbethegoaloftherapy?
8. Whenshouldwestartimmunosuppressivetherapy?Whichbiomarkersare
usefulinpredictingresponsetotherapy?Iskidneybiopsyusefulaspredictor?
9. Howshouldonemonitorpatientswhohavedevelopedremissionandwhichparametersshouldbeusedtoguiderestartofimmunosuppression?
10. Howshouldonedifferentiatebetweenproteinuriaduetorelapseorsecondaryfocalsegmentalglomerulosclerosis(FSGS)?
11. Howshouldtreatmentresistancebedefined(i.e.,non-responsiveness)?Whataretreatmentoptionsforinitiallynon-responsivepatients?Istherearoleforplasmaexchange(PLEX)?
12. AretherenewtreatmentoptionsdevelopedforuseinMN?ArethererandomizedclinicaltrialsorlargecomparativecohortstudiesinMNpublished
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after2010andhowshouldtheresultschangeKDIGOtreatmentguideline?WhatwillbetheimpactoftheMENTORandSTARMENstudies?
13. ShouldtreatmentbedifferentinpatientswithMNandimpairedkidneyfunction?Whatarepotentialthresholds?
14. Howshouldtreatmentbeadaptedinspecialpopulationssuchasinchildrenandpregnantwomen?
15. HowshouldwemanageMNpatientswhoreceiveakidneytransplant?WhatistheroleofaPLA2Rabbeforeandaftertransplantation?
Futurestudies16. WhatisthefutureofclinicaltrialsinMN?
• Inclusionofhigh-riskpatientsonly?• Appropriateendpoints?• Determiningoptimaltimeforassessingprimaryendpoint
Durationofclinicaltrial/follow-up• Patientreportedoutcomemeasures&sideeffects• OthermethodologybesidesRCTs.
Group4:Minimal-ChangeDisease(MCD)andFocalSegmentalGlomerulosclerosis(FSGS)Diagnosis,biomarkers&predictionofprognosis1. ShouldFSGSstillbeconsideredasinglediseaseentityorratherafamilyof
diseases?Canparticularsubsetsbeidentified?a. Shouldweabandon“Primary”and“Secondary”FSGSterminology?b. ArethetermsSSNSandSRNSstillrelevant?
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2. AretherenewinsightsintopathogenesisthatcanguidetreatmentinMCD,inparticularwithrespecttopermeabilityfactors?
3. WhatistheroleofgenetictestinginFSGS?Towhomandwhenshoulditbeapplied?Doesgenetictestinghelpinchoiceoftherapy?
4. Ishistologicalanalysisofrenaltissuesufficientfordiagnosisandmanagement
ofFSGSorshouldmoleculardiagnosisbeincorporatedintotheroutineevaluationofthebiopsytobetterdefinethevariantsthatcomprisethissyndrome?a. DothemorphologicalpatternsofFSGSbylightmicroscopyhavearolein
patientcare?b. ShouldwerecommendbiopsystandardsforFSGS?(i.e.,minimumnumberof
glomerulitoexcludeFSGSandwhoshouldbere-biopsied?)
Treatment5. WhoshouldreceiveimmunosuppressivetreatmentforFSGSandwhoshould
not?Ifneeded,whatisthemostreasonableimmunosuppressiveapproachwhencorticosteroidshavefailed?
6. Regardingimmunosuppression:a.WhenshouldtherapywithcalcineurininhibitorsorcytotoxicagentsbeconsideredinMCD?
b.Whatabouttherapywithrituximab,mycophenolatemofetil,adrenocorticotropichormone(ACTH)orabatacept?
c.Wouldoneofthesetherapiesbeusedasfirstlineinsteadofcorticosteroids?
d.WhatistheroleofplasmapheresisinFSGS?
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7. Regardinganti-proteinuricagents:a. Howdoweorshouldwedistinguishimmunosuppressivefromanti-proteinuriceffectsoftherapies(e.g.,steroids,cyclosporine,rituximab,ACTH)
b.WhatistheroleofangiotensinII/endothelinantagonisminallformsofFSGS?
8. Aretherenewinsightsintohowweshouldfollowandmanagetransplanted
patientswithahistoryofFSGS?Howshouldweapproachtreatmentofrecurrentdisease?
9. Whatarespecificaspectsregardingthecareforpediatricpatients?10. Whatarespecificaspectsregardingthecareforpregnantpatients?Futurestudies
11.WhatisthefutureofclinicaltrialsinMCD/FSGS?
• Doesitstillmakesensetostudy“FSGS”independentofthespecificentity?
• Inclusionofhigh-riskpatientsonly?• Appropriateendpoints?• Determiningoptimaltimeforassessingprimaryendpoint
Durationofclinicaltrial/follow-up• Patientreportedoutcomemeasures&sideeffects
Group5:Lupusnephritis(LN)andANCAvasculitis
Diagnosis,biomarkers&predictionofprognosis1. Whatistheroleofrepeatingthebiopsy,whenshoulditbedone,andhowoften?
IstherearoleforprotocolbiopsiesinthemanagementofLN?Howshouldwe
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bestusethekidneybiopsyinrelapsingdiseases?
2. Issimplehistology(light,immunofluorescence,andelectronmicroscopy)ofrenaltissuesufficientfordiagnosisandmanagementofheterogeneousdiseasesorshouldmoleculardiagnosisbeincorporatedintotheroutineevaluationofthebiopsy?IsthecurrentISN/RPSclassificationofLNsufficient?
3. Areproteinuria,urinarysedimentanalysisandSCroreGFRsufficienttodetermineresponsetotherapy?Whichcriteriashouldweusetodefineresponsetotreatment?Whatabouttheuseofdrugssuchascalcineurininhibitorsthatmayalterproteinuriabyseveralmechanisms?
4. a)Howcanwebestapplymyeloperoxidase(MPO),proteinase3(PR3)forpredictingrelapseinANCAvasculitis?Areimmune-enzymaticmethodsequivalenttoIFmethodswhentestingforANCA?Arethereotherpredictivebiomarkersthatshouldbeincorporatedintoclinicaluse,includingtherapy-specificbiomarkerssuchasB-cellcountsinpatientstreatedwithanti-Bcelltherapies?b)Howcanwebestapplyanti-DNA,complementandextractablenuclearantigen(ENA)profiletestingforpredictingrelapseinLN?Arethereotherpredictivebiomarkersthatshouldbeincorporatedintoclinicaluse,includingtherapy-specificbiomarkerssuchasB-cellcountsinpatientstreatedwithanti-Bcelltherapies?Whichapproachtoconsiderinserologicalactive(lowcomplementand/orpositiveanti-DNA)butclinicalsilentLNpatients?
5. Arethereanyclinicalsignsorserum/urinebiomarkers/geneticteststhatcanhelpto:a.predictwhomaydevelopkidneyinvolvementamongpatientswithsystemicANCAand/orhelpdiagnoseanddirecttherapy?b.predictwhomaydevelopLNamongpatientswithsystemiclupuserythematosus(SLE)and/orhelpdiagnoseanddirecttherapy?
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Treatment
6. AreweusingtoomuchcorticosteroidinLNandANCAvasculitis?Canwereducecumulativedosing?Areshortcourseofintravenouspulsesteroidssuperiortoprolongeduseoforalsteroids?
7. a.Forhowlongshouldmaintenancetherapybecontinuedinvasculitis?Whenshouldoneconsidertherapydiscontinuation?ShouldMPOandPR3positivepatientsreceivedifferentmaintenanceregimens?Dopatientswithdrug-inducedANCAvasculitisrequiremaintenance?b.ForhowlongshouldmaintenancetherapybecontinuedinLN?Howcanpatientcharacteristics(e.g.,responsetotherapy,historyofrelapse,biomarkersofdiseaseactivity)guidelengthofmaintenancetherapy?Whenshouldoneconsidertherapydiscontinuation?
8. HowshouldrefractorydiseaseinLNandANCAvasculitisbedefined?Whatstrategiesmaybeusedtotreatrefractorydisease?DoesinductiontherapydifferinpatientswithANCAvasculitiswhendiffusealveolarhemorrhageispresentand/ rapidlyprogressiverenalinsufficiency?
9. Whichistheroleofanti-BcellandotherbiologicaltherapiesinANCAvasculitisandLN?Whentoconsideranti-BcelltherapyinclassVLN?WhatistheroleofplasmaexchangeincrescenticANCAvasculitis?WhatistheroleofcomplementinhibitioninANCAvasculitisandLN?
10. Whichistheroleofantiphospholipidantibodies(aPL)testinginthecontextofLN?DoaPLandaPL-relatednephropathyhaveanimpactonthemanagementofLN?IfthromboticmicroangiopathyiscoexistentwithLNonkidneybiopsy,whatistheappropriateworkupandtreatment?Whatistheroleofplasmaexchange?Anticoagulation?Anti-complementtherapies?
11. WhatistheroleofCNIor“multi-targettherapy”inthetreatmentofLN?WhentoconsidertostopCNI?
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12. HowshouldLNbemanagedduringpregnancy? Whentoconsideranti-plateletagents?
13. HowshoulddiseaserecurrenceforLN/ANCAvasculitisbemanagedpost-transplant?
Futurestudies
14.WhatisthefutureofclinicaltrialsinSLE/ANCAvasculitis?
• Doesitmakesensetostudyparticularsubgroups?(e.g.,separatingMPOfromPR3;separatingclassVfromClassIII/IVLN)?
• Inclusionofhigh-riskpatientsonly?• Appropriateendpoints?• Determiningoptimaltimeforassessingprimaryendpoint• InclusionofpediatricpatientsinLNtrials• Durationofclinicaltrial/follow-up• Patientreportedoutcomemeasures&sideeffects
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